Relationship Between Activated Clotting Time and Ischemic or Hemorrhagic Complications: Analysis of 4 Recent Randomized Clinical Trials of Percutaneous Coronary Intervention

doi:10.1161/01.CIR.0000139868.53594.24

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Circulation. 2004;110:994-998
Published online before print August 9, 2004, doi: 10.1161/01.CIR.0000139868.53594.24

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(Circulation. 2004;110:994-998.)
© 2004 American Heart Association, Inc.

Original Articles

Relationship Between Activated Clotting Time and Ischemic or Hemorrhagic Complications

Analysis of 4 Recent Randomized Clinical Trials of Percutaneous Coronary Intervention

Sorin J. Brener, MD; David J. Moliterno, MD; A. Michael Lincoff, MD; Steven R. Steinhubl, MD; Kathy E. Wolski, MS; Eric J. Topol, MD

From the Department of Cardiovascular Medicine (S.J.B., A.M.L., K.E.W., E.J.T.), Cleveland Clinic Foundation, Cleveland, Ohio, and Divisions of Cardiology, University of Kentucky (D.J.M.), Lexington, Ky, and University of North Carolina (S.R.S.), Chapel Hill, NC.

Correspondence to Sorin J. Brener, MD, Assistant Professor of Medicine, Director, Angiography Core Laboratory, 9500 Euclid Ave, Desk F-25, Cleveland, OH 44195. E-mail breners{at}ccf.org

Received December 16, 2003; de novo received February 25, 2004; revision received April 20, 2004; accepted April 21, 2004.

Background— Unfractionated heparin (UFH) is the most widelyused antithrombin during percutaneous coronary intervention(PCI). Despite significant pharmacological and mechanical advancementsin PCI, uncertainty remains about the optimal activated clottingtime (ACT) for prevention of ischemic or hemorrhagic complications.

Methods and Results— We analyzed the outcome of all UFH-treatedpatients enrolled in 4 large, contemporary PCI trials with independentadjudication of ischemic and bleeding events. Of 9974 eligiblepatients, maximum ACT was available in 8369 (84%). The medianACT was 297 seconds (interquartile range 256 to 348 seconds).The incidence of death, myocardial infarction, or revascularizationat 48 hours, by ACT quartile, was 6.2%, 6.8%, 6.0%, and 5.7%,respectively (P=0.40 for trend). Covariate-adjusted rate ofischemic complications was not correlated with maximal proceduralACT (continuous value, P=0.29). Higher doses of UFH (>5000U, or up to 90 U/kg) were independently associated with higherrates of events. The incidence of major or minor bleeding at48 hours, by ACT quartile, was 2.9%, 3.5%, 3.8%, and 4.0%, respectively(P=0.04 for trend). In a multivariable logistic model with aspline transformation for ACT, there was a linear increase inrisk of bleeding as the ACT approached 365 seconds (P=0.01),which leveled off beyond that value. Increasing UFH weight-indexeddose was independently associated with higher bleeding rates(OR 1.04 [1.02 to 1.07] for each 10 U/kg, P=0.001).

Conclusions— In patients undergoing PCI with frequentstent and potent platelet inhibition use, ACT does not correlatewith ischemic complications and has a modest association withbleeding complications, driven mainly by minor bleeding. Lowervalues do not appear to compromise efficacy while increasingsafety.

Key Words: angioplasty • heparin • ischemia • hemorrhage

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